Tertiary amine methacrylate-based macromonomers and polymers

ABSTRACT

Compounds of general formula (I), the described methods to prepare these macromonomer compounds, and the copolymer products of these compounds with other vinyl monomers. Wherein W is a capping group; l is 0 or 1; n is 2-1000; m is 2-5; R 1  is CH 2 ═CH—CH 2 —, or CH 2 ═CH—O—R 8 —; R 2  is selected from H, CH 2 ═CH—CH 2 —, and phenyl or alkyl and wherein R 3 -R 7  is H 1 , C 1 -C 4  alkyl, and quaternary salts thereof. When R7 and X— is absent, the polymer is amphiphilic. When R7 is alkyl and X— is an anion, the polymer is cationic polymer.

FIELD OF THE INVENTION

This invention relates to tertiary amine methacrylate-based macromonomers and quaternary salts thereof; particularly macromonomers of dialkyl aminoethyl methacrylates with diallylalkylammonium or allylalkyl phenyl ammoniun or vinyloxypropyl terminal groups, polymers made therefrom and methods of preparation thereof.

BACKGROUND TO THE INVENTION

Random copolymers of cationic monomers with acrylamide are widely used to improve fines and filters retention during paper manufacture and sludge dewatering in newsprint deinking plants, as well as many other applications in mineral processing, oil recovery, and drinking water treatment.¹ Recently, it was demonstrated that graft copolymers, in which cationic units were concentrated on pendant chains, gave an much improved performance over their corresponding random polymers.^(2,3) However, these graft copolymers were synthesized by a gamma radiation-initiated graft copolymerization. It was very difficult to control the copolymerization and almost impossible to completely analyze the copolymer structure. e.g. the length of grafted side chain and graft density. Copolymerization of acrylamide with cationic macromonomers provides a good approach to prepare such copolymers with required chain length and side chain density by controlling the chain length and charged amount of a macromonomer. Therefore the cationic macromonomer precursors need to be synthesized first.

Tertiary dialkylaminoethyl methacrylate based polymers can easily be converted to cationic polymers by quaternization of the tertiary amine. These cationic polymers are very useful in wastewater treatment and papermaking industries. Therefore, the synthesis of well-defined DMAEMA macromonomers with polymerizable terminal unsaturated group is of both industrial and academic interests.

Macromonomers with polymerizable vinyl terminal group are usually synthesized by end-group functionalization of pre-polymers and chain transfer radical polymerization catalyzed by cobalt compounds. Main problems for these methods are that usually not all of the end groups can be functionalized and the resulting polymers have broad molecular weight distribution.

The initiation method using vinyl-containing initiators is an effective alternative approach to the preparation of well-defined macromonomers with narrow molecular weight distributions. The advantage of this method is that each polymer chain has a terminal vinyl group. The application of the initiation method in the synthesis of poly(meth)acrylate macromonomers is still very limited because it is difficult for an initiator such as alkyllithium to bear an unsaturated group.⁴ Recently, Nagasaki⁵ and Lascelles⁶ synthesized poly(diethylaminoethyl methacrylate) (polyDEAEMA) and poly(dimethylaminoethyl methacrylate) (polyDMAEMA) macromonomers with polymerizable terminal vinyl groups by using less active oxyanionic initiators. However, the molecular weights of the prepared polymers were higher than predicted and the polymer dispersities were about 1.3.

REFERENCES

1 Bolto, B. A. Prog. Polym. Sci. 1995, 20, 987

2 Ma, M., Zhu, S. Colloid Polym. Sci. 1999, 277, 123

3 Subramanian, R., Zhu, S., Pelton, R. H. Colloid Polym. Sci. 1999 to appear.

4 Jerome, R., Teyssie, Ph., Vuillemin, B., Zundel, T., Zune, C. J. Polym. Sci. Polym. Chem. 1999, 37, 1

5 Nagasaki, Y., Sato, Y., Kato, M. Macromol. Rapid Commun. 1997, 18, 827

6 Lascelles, S. F., Malet, F., Mayada, R., Billingham, N.C., Armes, S. P. Macromolecules. 1999, 32, 2462

SUMMARY OF THE INVENTION

The invention in one aspect provides compounds of the general formula I

wherein W is a capping group; l is or 1; n is 1-1000; m is 1-5; preferably m is 2;

R₁ is selected from CH₂═CH—CH₂— and CH₂═CH—O—(CH₂)_(p)—; p is 1-5;

R₂ is selected from H, CH₂═CH—CH₂—, and phenyl

and wherein R₃-R₅ is C₁-C₄ alkyl, and quaternary salts thereof wherein R₆ is C₁-C₄ alkyl and X⁻ is an anion.

Preferably, m is 2 when R₃ is CH₃.

When amphiphilic macromonomers are needed, R₄-R₅ are C₁-C₄ alkyls and R₆ is absent to thus represent non-quaternized macropolymers.

When cationic macromonomers are desired, R₄-R₆ are C₁-C₄ alkyls, and complementary X are present.

Most preferably, n is selected from 5-200 and, still further preferred, n is 10-100.

Water-soluble cationic macromonomers of dialkylaminoalkyl methacrylate with polymerizable diallylmethylammonium or allylmethylphenylammonium or vinyloxyalkyl terminal groups embodiments of the aforesaid compounds according to the invention were synthesized by N-substituted amine—butyllithium (BuLi) initiated anionic polymerization of dialkylaminoalkyl methaerylate, particularly, DMAEMA and subsequent quaternization. We found that diallylamine-BuLi initiated a living polymerization. The resulting polymers had a very narrow molecular weight distribution with initiator efficiency about 0.25. The initiator efficiency of allylphenylamine-BuLi was as high as 0.63. A capping method was thus developed to improve the initiator efficiency of dilallylamine-sBuLi system. Capped with dimethylacrylamide (DMA) or tert-butyl methacrylate (tBMA), the initiation efficiency of the diallylamine-sBuLi system was increased to a level as high as 0-95. Similarly, DMA-capped vinyloxypropylamine-sBuLi had about 0.6 initiator efficiency, but its uncapped system could not initiate the polymerization. The polymerization produced amphiphilic macromonomers with predictable molecular weight and extremely low polydispersity. The quaternization of the polymers with CH₃I and dimethyl sulfate gave corresponding cationic macromonomers with diallylmethylammonium or allylmethylphenylammonium, or vinyloxypropyl end groups, which were readily polymerizable by free radical polymerization mechanism.

Thus, in one aspect of the invention provides the synthesis and characterization of cationic macromonomers with diallylmethylammonium or allylmethylphenyl ammonium or vinyloxypropyl terminal group by a living polymerization of DMAEMA. These vinyl groups are active double bonds for the copolymerization with water-soluble monomers such as acrylamide or other organic soluble monomers such as methymethacrylate (MMA) and styrene (St) to make amphiphillic copolymers

Thus, the present invention in one aspect provides polyDMAEMA macromonomers with polymerizable terminal vinyl groups synthesized by a living anionic polymerization with N-substituted amine-butyllithium initiator system. We have found that the alkylamine substituent had a strong effect on the initiator efficiency in the order of H<allyl<phenyl. We have found that the capping of diallylaminolithium with dimethylacrylamide or t-butylmethacrylate gave high initiator efficiencies and an excellent control of the molecular weight. Still further, we have also found that a one to three-fold LiCl with respect to the initiator gave polyDMAEMA with controlled molecular weight and narrow molecular weight distribution. However, too excess LiCl reduced the initiator efficiency. We have also found that the quaternization of terminal diallylamino and allylphenylamino groups required a strong methylizating agent such as (CH₃)₂SO₄, while the dimethylamino group in the polymer chain was quaternized by CH₃I.

We have found that lithium amides prepared from primary amine-BuLi could not initiate the polymerization of DMAEMA. However, when these lithium amides were capped with dimethylacrylamide (DMA), named as capping agent, they could initiated the DMAEMA polymerization and yielded polymers with narrow molecular weight distribution. Thus the invention also provides the synthesis of amphiphilic and cationic macromonomers of DMAEMA with the terminal vinyl or allyl group by the living DMAEMA polymerization initiated by capped primary amine-BuLi systems. Further, we have found that vinyl-terminated poly(DMAEMA) and its corresponding cationic macromonomers or diallylmethylammonium terminated cationic macromonomers are readily copolymerizable with other vinyl monomers such as styrene and acrylamide, while allyl-terminated macromonomers are versatile for further modification, for example, hydrosillation, transformation with epoxy and hydroxyl groups, and synthesis of block and graft copolymers.

BRIEF DESCRIPTION OF THE DRAWINGS

In order that the invention may be better understood preferred embodiments will now be described by way of example only, with reference to the accompanying drawings wherein:—

FIG. 1 is a gel permeation chromatography (GPC) scan showing GPC traces of polyDMAEMA initiated by diallylamine-sBuLi: (a) Table 1 entry 6 and (b) Table 1 entry 4;

FIG. 2 is a GPC scan showing GPC traces of polyDMAEMA initiated by DMA-capped diallylaminolithium: (a) without LiCl (Table 2 entry 1), (b) with 3-fold LiCl (Table 2 entry 3), and (c) with 10-fold LiCl (Fable 2 entry 8);

FIG. 3 is a nuclear magnetic resonance (NMR) scan showing ¹H-NMR spectra of polyDMAEMA macromonomers prepared by (a) diallylamine-sBuLi and (b) allylphenylamine-sBuLi;

FIG. 4 is a NMR scan showing ¹H-NMR spectra of quaternized polyDMAEMA macromonomers: (a) diallylamino-terminated polyDMAEMA reacted with CH₃I at room temperature for 1 h, (b) diallylamino-terminated polyDMAEMA reacted with (CH₃)₂SO₄ in DMSO for 1 h, (c) allylphenylamino-terminated polyDMAEMA reacted with (CH₃)₂SO₄ in DMSO for 6 h; and

FIG. 5 represents a flocculation test graph showing relative turbidity against time.

DETAILED DESCRIPTION OF PREFERRED EMBODIMENTS

Experimental Section

Reagents and Solvents

Dimethylaminoethyl methacrylate (DMAEMA) from Aldrich was stirred over CaH₂ for 24 h, then was distilled from CaH₂ under a reduced pressure and stored under nitrogen in a refrigerator. LiCl (99.9%) from Aldrich was dried at 130° C. and then dried again at 100° C. under vacuum just before use. THF was refluxed over potassium under nitrogen atmosphere. Diallylamine, allylamine and allylaniline were distilled over CaH₂. Secondary-butyllithium (sBuLi) was purchased from Aldrich and its concentration was titrated by a standard method. 3-Aminopropyl vinyl ether (AVE) (Aldrich), aminostyrene (AS) (Alfa Aser) and allylamine (AA) (Aldrich) were dried and distilled over CaH₂.

Preparation of Initiator and Polymerization

In a glass reactor previously treated with chlorotrimethylsilane and flame dried, weighted LiCl was added and heated to 100° C. under vacuum and purged with nitrogen 5 times. Then 30 ml THF and required amount of N-substituted allylamine were charged to the reactor. The reactor was cooled down to −78° C. A stoichiometric amount of s-butyllithium was added dropwisely with stirring. After 1 h of stirring, the monomer was introduced. In the runs with a capping agent, 2-fold (molar) dimethylacrylamide or tert-butyl methacrylate with respect to N-substituted allylamine was introduced and stirred at −78° C. for 0.5 h before adding monomer. The polymerization was terminated by adding 0.2 ml methanol. The aliquot was then poured into 200-ml petroleum ether. Finally the polymer was separated and dried in vacuum at 30° C. for 24 h.

Quaternization of the Polymers

1 g polymer was dissolved in 10 ml acetone or DMSO or dimethylforamide (DMF) at room temperature. 0.5 ml CH₃I was then added dropwisely and stirred for 2 h. 0.1 ml dimethyl sulfate was then added and the solution was stirred for another hour. When using acetone as solvent, the quaternized polymer precipitated very quickly after adding CH₃I. The precipitate was isolated and dried in the vacuum oven. When DMSO or DMF was used as solvent, the quaternized polymer was soluble in DMSO and therefore the reaction in DMSO or DMF was homogenous The quaternized polymer was precipitated in acetone and also dried in vacuum.

Characterization

Nuclear Magnetic Resonance (NMR) Spectroscopy: Proton (¹H) NMR spectra were recorded on a Bruker ARX-200 spectrometer at 200 MHz. ¹H NMR chemical shifts in CDCl₃ were reported downfield from 0.00 ppm using CHCl₃ signal at 7.23 ppm as an internal reference. When D₂O was used as solvent, H₂O signal at 4.63 ppm was used as reference.

Molecular Weight Measurements: Number and weight average molecular weights (M_(n) and M_(w), respectively) were determined by gel permeation chromatography (GPC) using THF-2% (v/v) trimethylamine as eluent at 25° C. with RI detector. Narrow polystyrene standards (Polysciences) were used to generate a calibration curve (Varian MicroPak column G1000, 3000, 7000 HXL). Data were recorded and processed using the Windows based Millenium 2.0 software package.

Results

1. DMAEMA Polymerization by N-Substituted Allylamine-sBuLi Initiator System

The initiator, N-substituted allylaninolithium, was prepared in-situ by the reaction of N-substituted allylamine with s-butyllithium (see Scheme 1). The effects of experimental conditions for the initiator preparation and polymerization were summarized in Table 1. If both the initiator preparation and polymerization of DMAEMA were carried out at 0° C., the polymerization gave only 33% polymer (Table 1, entry 1). If the initiator was prepared at 0 or 25° C. while the polymerization was carried out at −78° C., the conversion was almost complete, but the molecular weight of the resulted polymer deviated far from the predicted (Table 1, entries 2 and 3). The initiation efficiency (the ratio of calculated Mn over measured Mn) with respect to diallylamine was about 15% only.

TABLE 1 Synthesis of PDMAEMA macromonomers by living polymerization of DMAEMA initiated by alkylamine/s-butyllithium in the presence of Lithium chloride Reaction Polym. LiCl/ DA/ Conv. Calculated Mn Run Init. Temp. (° C.) Temp. (° C.) BuLi BuLi (%) DP (GPC) Efficiency Mw/Mn 1 DA 0 0 10 1 33 1884  3500 — 1.11 2 DA 25 −78 10 1 99 4700 32700 0.16 1.09 3 DA 0 −78 10 1 98 4700 29000 0.14 1.10 4 DA −78 −78  0 1 99 4700 17200 0.27 2.49 5 DA −78 −78  1 1 99 4700 19000 0.24 1.07 6 DA −78 −78  3 1 98 4700 18800 0.25 1.08 7 DA −78 −78 10 1 99 4700 19000 0.24 1.05 8 DA −78 −78  1 10  98 4700 19600 0.24 1.04 9 DA −78 −78 10 10  97 9600 24600 0.39 1.02 10  DA −78 −78 10 10  97 12700  36600 0.35 1.02 11  AAM −78 −78 10 10  98 5024  8000 0.63 1.11 12  AAn −78 −78 10 10   0 — — — — [alkylaminolithium] = 0.017 mol/L; DA = diallylamine; AAM = allylamine; AAn = allylaniline

When both the initiator preparation and successive polymerization were carried out at −78° C., the initiator efficiency increased to about 25% as shown in Table 1. The corresponding GPC trace (FIG. 1, a) shows a unimodal with extremely narrow molecular weight distribution. This result indicates that the initiation reaction was very fast and that once a polymer chain started to propagate, there was no side reaction of the polymer anion. Furthermore, the amount of added LiCl had some effect on the polymerization. In the absence of LiCl, the polymerization produced polymer with very broad molecular weight distribution (Mw/Mn=2.49) (FIG. 1b). But in the presence of LiCl, the polymer appeared to be nearly monodispersed (Table 1, entries 5-7) (FIG. 1a). It seems that the presence of LiCl suppressed side reactions of the living polymeric carbanion attacking the carbonyl groups in the polymer and monomer.⁴ However, the presence of LiCl did not increase the initiation efficiency. With or without LiCl, the initiation efficiencies of diallylamine were about 0.25.

The effect of added amount of diallylamine was also investigated. Interestingly, the presence of excessive diallylamine did not decrease the molecular weight of polyDMAEMA, as shown in Table 1 entry 8. Given the same concentration of s-butyllithium (compared to entry 5), the molecular weight of polyDMAEMA remained unchanged and the molecular weight distribution of prepared polyDMAEMA was still narrow, regardless of the amount of added diallylamine. This indicates that the formed carbanions did not abstract the N—H hydrogen on diallylamine (Scheme 2). Thus, sBuLi can be allowed to react with an excess amount of diallylamine to minimize side reactions of sBuLi during the initiator preparation.

Allylaniline (AAn) and allylamine (AAm) were also tested for the polymerization of DMAEMA to further investigate the effect of alkyl moiety on the initiator efficiency (Table 1, entries 11 and 12). When allylaninolithium (Scheme 3b), prepared by the reaction of allylamine with sBuLi, was used as initiator, no polymer was obtained, while allylphenylaminolithium (Scheme 3c), derived from the reaction of allylaniline with sBuLi, had much higher initiator efficiency, 0.63, than that of diallylaminolithium (Scheme 3a). Apparently, the structure of the nitrogen substituent influences the initiator efficiency. For N-substututed allylamines, the efficiency increased in the order of H<<allyl<phenyl.

2. Diallylamine/sBuLi-Capping Agent Initiated Polymerization of DMAEMA

In an effort to improve initiator efficiency, the diallylaminolithium was capped with dimethylacrylamide (DMA) and tert-butyl methacrylate (tBMA) and the polymerization results were summarized in Table 2.

TABLE 2 DMAEMA polymerization initiated by capped-diallylaminolithium at −78° C.^(a) Caaping DMAEMA/ Conv. Mn Mn Initiator Run agent LiCl ratio Solvent Solvent (%) Calcu. GPC Efficiency Mw/Mn 1 DMA 30 0 THF 99 4700 38300 0.12 2.89 2 DMA 30 1 THF 98 4700  5310 0.89 1.06 3 DMA 27 3 THF 99 4200  4440 0.95 1.04 4 DMA 40 3 THF 99 6280  6500 0.96 1.08 5 DMA 78 3 THF 98 12300  13700 0.90 1.08 6 DMA 150  3 THF 99 23300  25500 0.93 1.04 7 DMA 30 3 THF-Toluene^(b) 95 4700 24600 0.19 4.86 8 DMA 30 10  THF 99 4700  9600 0.49 1.06 9 DMA 60 10  THF 100  9420 15000 0.63 1.08 10  tBMA 30 3 THF 99 4700  4900 0.96 1.03 11  tBMA 50 3 THF 99 7800  8300 0.94 1.05 12  tBMA 64 3 THF 99 10000  11500 0.87 1.07 13  tBMA 60 10  THF 97 9420 17000 0.55 1.04 14  MAN 30 3 THF 100  4700 19500 0.21 1.31 ^(a)[Diallylaminolithium] = 0.017 mol/L, ^(b)Toluene/THF = 9/1 (v/v).

The results in Table 2 show that DMA or tBMA-capped diallylaminolithium had very high activities. The monomer conversions were almost complete. More importantly, the molecular weights of the obtained polymers agreed with the calculated ones and the initiator efficiencies were as high as 0.95 in the presence of 3-fold LiCl (Table 2, entries 26, 10-12). The molecular weight distributions were very narrow with dispersities below 1.1. These results suggest that there were essentially no chain transfer and termination reactions. This assured that each polymer chain had one initiator terminal group, which is very important for the macromonomer.

The high efficiencies of the capped diallylaminolithium indicated a complete capping reaction. The narrow GPC traces of the resulting polymers (FIGS. 2b, c) demonstrated that there was only a single type of initiation center. It can be postulated that either diallylaminolithium did not strongly associate or it disassociated into monomeric structure in the presence of LiCl. This conclusion was confirmed by the diallyaminolithium-initiated homopolymerization of tBMA, in which high initiator efficiencies were also obtained. The low efficiency in the diallylaminolithium-initiated polymerization of DMAEMA was attributed to the reaction of diallyaminolithium with the monomer carbonyl group.

The LiCl amount in the polymerization system had a dramatic effect of the DMAEMA polymerization initiated by the capped diallylaminolithium. Without LiCl, DMA-capped diallylaminolithium had a very low initiation efficiency (Table 2 entry 1), and the polymer had a broad molecular weight distribution (FIG. 2a). However, adding 1 or 3-fold LiCl substantially increased the initiator efficiency up to 0.95 and yielded polymers with extremely narrow molecular weight distributions (Table 2 entries 2-6) (FIG. 2b). By contrast, the presence of LiCl did not improve the initiator efficiency of the uncapped diallylaminolithium (Table 1).

Very high LiCl addition had a detrimental effect on the initiation efficiency for both DMA and tBMA-capped diallylaminolithium (Table 2, entries 8, 9, 13). For example, the efficiencies of the capped diallylamino lithium decreased to about 0.5 with a 10-fold LiCl. This effect of excess LiCl may be due to the fact that there are too many LiCl molecules surrounding an initiator anion. Some initiators thus become dormant in clusters and inactive in the initiation of DMAEMA. We also tested toluene/THF (9:1 v/v) as a solvent and found low initiator efficiency and very poor control of molecular weight (Table 2 entry 7).

3. The DMAEAM Polymerization with Primary Amine-sBuLi System

As stated above, the primary amine-sBuLi without capping could not initiate DMAEMA polymerization. Table 3 also shows that the three primary amine-BuLi systems, AVE-BuLi, AS-BuLi and AA-BuLi, (Table 1, entries 1-3) could not initiate the DMAEMA polymerization.

TABLE 3 Synthesis of PDMAEMA macromonomers by living polymerization of DMAEMA initiated by primary amine-butyllithium in the presence of Lithium chloride. Run Alkylamine Cap agent LiCl/BuLi Conv. (%) Mn (Calculated) Mn (GPC) I. E. Mw/Mn 1 AVE — 3  0 — — 0 — 2 SA — 3  0 — — 0 — 3 AA — 3  0 — — 0 — 4 AVE tBMA 3 99 4900 25500 0.19 1.23 5 AVE DMA 3 98 2555  4700 0.54 1.14 6 AVE DMA 3 98 4900  8600 0.57 1.11 7 AVE DMA 3 99 5200  9300 0.56 1.10 8 AVE DMA 3 98 9620 16800 0.57 1.12 9 AVE DMA 0 100  4900 39200 0.13 2.75 10  AVE DMA 10  95 4900 15013 0.33 1.14 11  AVE DMA 10  97 4900 11000 0.44 1.13 12  AVE DMA 10  96 9620 25300 0.38 1.09 13  AA DMA 3 99 2800  4750 0.59 1.09 14  AA DMA 3 99 4900  8000 0.61 1.13 15  AA DMA 3 100  6480 10550 0.61 1.08 16  SA DMA 3 99 4900 17100 0.28 1.23 −78° C. in THF

When tBMA was used as a capping agent, the capped AVE-BuLi could initiate the DMAEMA polymerization with near 100% conversion. However, the molecular weight of the resulted polymers was much higher than the predicated. The initiation efficiency of the tBMA-capped AVE-BuLi was only as low as 0.19. This was much lower than tBMA-capped diallylamine-BuLi system (initiator efficiency about 0.95) for the DMAEMA polymerization. By contrast, after being capped with DMA, AVE-BuLi and AA-BuLi initiator systems initiated a living polymerization of DMAEMA, yielding polymers with controlled molecular weight and low polydispersity, around 1.1. The molecular weights measured by GPC were about the half of the predicated. The initiator efficiencies of the capped AVE-BuLi and AA-BuLi systems were about 0.55.

4. Characterization of the Macromonomers

The macromonomers were characterized by ¹H-NMR. FIG. 3 shows the NMR spectrum of polyDMAEMA prepared by diallylamine-sBuLi. Signals of polyDMAEMA backbone are 2.25 ppm (N(CH ₃)₂), 2.55 (NCH ₂), 4.05 ppm (COOCH ₂), 1.65˜2.05 ppm (CH ₂—C—CH₃), 0.87 and 1.05 ppm (CH ₃—C). The double bond signals for diallylamino group appear at 5.1 ppm (multiple) (CH₂═) and 5.7 ppm (multiple) (═CH) (FIG. 3a), which are very similar to the signals of diallylamine. The signals of allyl group in allylphenylamino appear at up-field, 5.6 ppm (multiple) (═CH) and 5.05 ppm (multiple) (CH₂═), due to the conjugation of benzene ring with the nitrogen atom.

The obtained polymers were reacted with quaternization agents to prepare polymerizable cationic macromonomers. Two types of tertiary amino groups—pendant dimethylamino and terminal diallyamino or allylphenylammino group—need to be quaternized. The terminal diallylamino ((CH₂═CH—CH₂)₂N—) or allylphenylamino((CH₂═CH—CH₂N(C₆H₅)) group must be quaternized to make it polymerizable by free radical mechanism because un-quaternized diallylamine does not polymerize.²² It was found that these two types of amino groups had very different reactivities. The dimethylamino group is very easy to be quaternized by CH₃I at room temperature or by benzyl chloride at 40° C. For example, after 1 h reaction with CH₃I at room temperature, all the dimethylamino groups were converted into trimethylammonium ((CH₃)₃N⁺), as shown in FIG. 4. The signal for NCH ₃ at 2.25 ppm disappeared completely while a strong peak for N⁺CH₃ appeared at 3.20 ppm.

However, there was no change for the allyl peak form either diallylamino or allylphenylamino terminal group (FIG. 5a). Increasing the quaternization temperature or prolonging the reaction time of CH₃I or PhCH₂Cl could only partially quaternize these terminal groups. Unfortunately those more extreme conditions caused some double bonds disappear, which was possibly due to reaction with 12 generated from the decomposition of CH₃I.

The more powerful methylizating agent, (CH₃)₂SO₄, quantitatively quaternized both types of tertiary amino groups in the polymer. For example, after 1 h reaction in DMSO at room temperature, the terminal diallylamino group was completely quaternized, as seen in NMR spectra (FIG. 4b). The allyl proton signals at 5.1 ppm (CH₂═) and 5.7 ppm (═CH) shifted to 5.45 ppm and 5.70 ppm, respectively. The complete quaternization of allylphenylamino group with dimethyl sulfate required 6 h (FIG. 4c). This lower reactivity of allylphenylamino group may be due to the combination of high steric hindrance effect of the benzene ring and the conjugation of the nitrogen atom with benzene ring, which substantially decreases the electron density on the nitrogen atom.

5. Copolymerization with Acrylamide

Copolymerization of the quaternized macromonomer with acrylamide was conducted using AIBA as a radical initiator. 1 g (M_(n)=9000) of the macromonomer, 1 g of acrylamide, 5 mg of AIBA and 15 mL of water were charged to a tube reactor. The tube was degassed with argon for ten minutes and sealed with rubber septum. The tube was then immersed into a water bath at 60° C. After reaction for 4 h, the polymer was precipitated in methanol and dried in vacuum to yield 1.8 g of comb polymer with conversion 90% with respect to the total monomers charged.

FIG. 5 shows the improved flocculation properties of a comb-branched copolymer on a TiO₂ particulate aqueous suspension.

The acrylamide-co-DMAEMA macromonomer had a macromonomer content of 26% (A) and prior art random copolymer cationic unit content of 23%.

Although this disclosure has described and illustrated certain preferred embodiments of the invention, it is to be understood that the invention is not restricted to those particular embodiments. Rather, the invention includes all embodiments which are functional or mechanical equivalence of the specific embodiments and features that have been described and illustrated. 

What is claimed is:
 1. Compounds of the general formula I

wherein W is a capping group; l is 0 or 1; n is 1-1000; m is 1-5; R₁ is selected from CH₂═CH—CH₂— and CH₂═CH—O—(CH₂)_(p)—, p is 1-5; R₂ is selected from H, C₁-C₄alkyl, CH₂═CH—CH₂—, or phenyl; when R₁ is CH₂═CH—O—(CH₂)_(p), R₂ is H or C₁-C₄alkyl; and R₃-R₆ are C₁-C₄ alkyl; and quaternary salts thereof when R₆ is C₁-C₄alkyl and X is an anion.
 2. Compound as defined in claim 1 wherein m is 2 and R₃-R₆ is C₁-C₄ alkyl.
 3. Compound as defined in claim 1 wherein m is 2 and R₃ is CH₃.
 4. Compound of claim 1 wherein n is 5-200.
 5. Compound of claim 1 wherein n is 10-100.
 6. Compound of claim 1 wherein R₆ is CH₃.
 7. Compound as defined in any one of claims 1 to 6 wherein W is selected from

wherein R₇-R₁₁ is a C₁-C₄ alkyl.
 8. Method for preparing a macromonomer compound of the general formula II

wherein n is 1-100; l is 0, R₁ is CH₂═CHCH₂— or CH₂═CH—O—(CH₂)_(p); p is 1-5; m is 1-5; R₂ is selected from H; CH₂═CHCH₂—, phenyl; R₃-R₆ is C₁-C₄ alkyl; and W is selected from

wherein R₇-R₁₁ is a C₁-C₄ alkyl, comprising polymerizing a compound of the general formula III with a nitrogen anion IV


9. Method for preparing a macromonomer compound of the general formula II

wherein n is 1-100; l is 1, R₁ is CH₂═CHCH₂— or CH₂CH—O—(CH₂)_(p); p is 1-5; m is 1-5; R₂ is selected from H; CH₂=CHCH₂— and phenyl; R₃-R₆ is C₁-C₄ alkyl; and W is selected from

comprising polymerizing a nitrogen anion of the general formula IV

wherein R₇-R₁₁ is a C₁-C₄ alkyl to provide a compound selected from VII and VIII, respectively

and polymerizing said VII or VIII with a compound of the general formula III CH₂═CR₃COOR₄NR₅R_(6.)
 10. Method for the production of quaternized macromonomers of the general formula I wherein R₆ is present, comprising treating said macromonomer wherein R₆ is absent with a R₆ X quaternizing agent, and wherein the general formula I comprises

wherein W is a capping group; l is 0 or 1; n is 1-1000; m is 1-5; R₁ is selected from CH₂═CH—CH₂— and CH₂═CH—O—(CH₂)_(p)—, p is 1-5; R₂ is selected from H, C₁-C₄alkyl, CH₂═CH—CH₂—, or phenyl; when R₁ is CH₂═CH—O—(CH₂)_(p), R₂ is H or C₁-C₄alkyl; and R₃-R₆ are C₁-C₄ alkyl; and quaternary salts thereof when R₆ is C₁-C₄alkyl and X is an anion.
 11. Method comprising copolymerizing a macromonomer of the general formula I with vinyl monomers to prepare copolymers of general formula X, wherein l is 0 or 1, n is 1-1000, x and y are 10-1000; R₁ is CH₂—CH—O—R₉ or CH₂CH—CH₂, R₂ is H or C₁-C₄-alkyl; R₃-R₇ are C₁-C₄ alkyl; and R₈ is phenyl or ester, amide groups

and wherein the general formula I comprises

wherein W is a capping group; l is 0 or 1; n is 1-1000; m is 1-5; R₁ is selected from CH₂═CH—CH₂— and CH₂CH—O—(CH₂)_(p)—, p is 1-5; R₂ is selected from H, C₁-C₄alkyl, CH₂CH—CH₂—, or phenyl; when R₁ is CH₂CH—O—(CH₂)_(p), R₂ is H or C₁-C₄alkyl; and R₃-R₆ are C₁-C₄ alkyl; and quaternary salts thereof when R₆ is C₁-C₄alkyl and X is an anion.
 12. Method comprising copolymerizing said macromonomer of the general formula I with amphiphilic monomers to prepare water soluble copolymers of general formula XI, wherein l is 1-3, n is 1-1000, x and y are 10-1000; R₁ and R₂ is CH₂═CH—CH₂, R₃-R₇ are C₁-C₄ alkyl; R₈ is methyl; and R₉ is an amide group or NHC(O)H or any other hydrophilic groups

wherein the general formula I comprises

wherein W is a capping group; l is 0 or 1; n is 1-1000; m is 1-5; R₁ is selected from CH₂═CH—CH₂— and CH₂═CH—O—(CH₂)_(p)—, p is 1-5; R₂ is selected from H, C₁-C₄alkyl, CH₂═CH—CH₂—, or phenyl; when R₁ is CH₂═CH—O—(CH₂)_(p), R₂ is H or C₁-C₄alkyl; and R₃-R₆ are C₁-C₄ alkyl; and quaternary salts thereof when R₆ is C₁-C₄alkyl and X is an anion.
 13. Compound of claim 2 wherein n is 5-200.
 14. Compound of claim 3 wherein n is 5-200.
 15. Compound of claim 2 wherein n is 10-100.
 16. Compound of claim 3 wherein n is 10-100.
 17. Compound of claim 2 wherein R₆ is CH₃.
 18. Compound of claim 3 wherein R₆ is CH₃.
 19. Compound of claim 4 wherein R₆ is CH₃.
 20. Compound of claim 5 wherein R₆ is CH₃. 